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一种针对α-拉曲毒素的钙离子非依赖性受体(CIRL),通过多种机制介导对分泌的影响。

A Ca2+-independent receptor for alpha-latrotoxin, CIRL, mediates effects on secretion via multiple mechanisms.

作者信息

Bittner M A, Krasnoperov V G, Stuenkel E L, Petrenko A G, Holz R W

机构信息

Department of Pharmacology, The University of Michigan Medical School, Ann Arbor, Michigan 48109, USA.

出版信息

J Neurosci. 1998 Apr 15;18(8):2914-22. doi: 10.1523/JNEUROSCI.18-08-02914.1998.

Abstract

alpha-Latrotoxin (alpha-Ltx), a component of black widow spider venom, stimulates secretion from nerve terminals and from PC12 cells. In this study we examine the effects of expression of a newly cloned Ca2+-independent receptor for alpha-Ltx (CIRL) on secretion from bovine chromaffin cells. We first characterized the effect of alpha-Ltx on secretion from untransfected cells. alpha-Ltx, by binding in a Ca2+-independent manner to an endogenous receptor, causes subsequent Ca2+-dependent secretion from intact cells. The stimulation of secretion is correlated with Ca2+ influx caused by the toxin. In permeabilized cells in which the Ca2+ concentration is regulated by buffer, alpha-Ltx also enhances Ca2+-dependent secretion, indicating a direct role of the endogenous receptor in the secretory pathway. Expression of CIRL increased the sensitivity of intact and permeabilized cells to the effects of alpha-Ltx, demonstrating that this protein is functional in coupling to secretion. Importantly, in the absence of alpha-Ltx, the expression of CIRL specifically inhibited the ATP-dependent component of secretion in permeabilized cells without affecting the ATP-independent secretion. This suggests that this receptor modulates the normal function of the regulated secretory pathway and that alpha-Ltx may act by reversing the inhibitory effects of the receptor.

摘要

α-拉托毒素(α-Ltx)是黑寡妇蜘蛛毒液的一种成分,可刺激神经末梢和PC12细胞分泌。在本研究中,我们检测了新克隆的α-Ltx钙非依赖性受体(CIRL)的表达对牛嗜铬细胞分泌的影响。我们首先确定了α-Ltx对未转染细胞分泌的作用。α-Ltx以钙非依赖性方式与内源性受体结合,导致完整细胞随后发生钙依赖性分泌。分泌的刺激与毒素引起的钙内流相关。在通过缓冲液调节钙浓度的透化细胞中,α-Ltx也增强了钙依赖性分泌,表明内源性受体在分泌途径中起直接作用。CIRL的表达增加了完整细胞和透化细胞对α-Ltx作用的敏感性,表明该蛋白在与分泌偶联中起作用。重要的是,在没有α-Ltx的情况下,CIRL的表达特异性抑制了透化细胞中ATP依赖性分泌成分,而不影响ATP非依赖性分泌。这表明该受体调节调节性分泌途径的正常功能,并且α-Ltx可能通过逆转受体的抑制作用发挥作用。

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